FRI0548 EFFICACY AND SAFETY OF TOCILIZUMAB IN SYSTEMIC AND POLYARTICULAR JUVENILE IDIOPATHIC ARTHRITIS – DATA OF THE BIKER REGISTRY

Background Since 2011 Tocilizumab is approved for systemic juvenile idiopathic arthritis (JIA) and since 2013 for polyarticular JIA Objectives To describe efficacy and safety of Tocilizumab in clinical practice in polyarticular (pJIA) and systemic JIA (sJIA) patients using the German Biologics registry (BiKeR) Methods Baseline demographics and disease activity parameters have been documented. Efficacy was determined using the JADAS10 prospectively. Safety assessments were based on adverse events reports (AE) processed according to MedDRA Results Until October 1, 2018, 345 JIA patients treated with Tocilizumab were registered, representing 635 patient-years (PY) of observation. The cohort treated with Tocilizumab had experienced disease duration of 5.5+/-4.3 years (mean+/-SD) for sJIA and 5.9+/-4.1 years for pJIA. sJIA/pJIA patients received pretreatment with MTX 72%/96%, Anakinra 23%/1%, Adalimumab 4%/60%, Etanercept 30%/69%, Canakinumab 2%/0%. Concomitantly, sJIA/pJIA patients received NSAIDs 64%/57%, systemic steroids 72%/35%, MTX 55%/54%, other DMARDS 4%/8%. At last follow-up, 63%/60%/51%/43% of sJIA and 56%/49%/40%/30% of pJIA patients reached JIAACR30/50/70/90 criteria. After 2 years of treatment JADAS remission was reached by 50%/43% and JADAS minimal disease activity by 67%/67%. 586 AE were reported during exposure plus 90 days of observation. The rate was significantly higher in sJIA (104/100PY [95% CI 92-119]) than in pJIA patients (79 [79-90]; RR 1.3; p=0.003). 75 qualified as serious AE (SAE) with a higher rate in sJIA (22[16-29] vs. 8 [5-12], RR 2.6; p Conclusion The analysis adds to the established safety profile of tocilizumab in paediatric patients with systemic & polyJIA. Differences were noted between pJIA and sJIA cohorts, the latter with higher rates of total number of adverse events, serious AE, infections and cytopenias, probably due to higher doses or shorter application intervals. No new safety signals specific to the paediatric population were identified in this large cohort of JIA patients. References [1] Horneff G, et al. Arthritis Res Ther. 2016Nov24;18(1):272 Acknowledgement BIKER and the documentation of the treatment with biologics is partially sponsored by Chugai and Roche, Germany Disclosure of Interests Ariane Klein: None declared, Gerd Ganser: None declared, Ralf Trauzeddel: None declared, Kisten Minden Grant/research support from: Pfizer, Abbvie, Christoph Rietschel: None declared, Jasmin Kuemmerle-Deschner Grant/research support from: Jasmin Kuemmerle-Deschner is an employee of University of Tuebingen, Germany, and received consultants/speakers fees from Novartis and SOBI pharmaceuticals and grant support from SOBI and Novartis., Consultant for: Jasmin Kuemmerle-Deschner is an employee of University of Tuebingen, Germany, and received consultants/speakers fees from Novartis and SOBI pharmaceuticals and grant support from SOBI and Novartis., Speakers bureau: Jasmin Kuemmerle-Deschner is an employee of University of Tuebingen, Germany, and received consultants/speakers fees from Novartis and SOBI pharmaceuticals and grant support from SOBI and Novartis., Gerd Horneff: None declared